Discovery of Terminal Oxazole‐Bearing Natural Products by a Targeted Metabologenomic Approach

恶唑 基因 放大器 生物 药物发现 生物化学 组合化学 聚合酶链反应 化学 立体化学
作者
Jiyoon Park,Yern‐Hyerk Shin,Sunghoon Hwang,Jung-Woo Kim,Dong Hyun Moon,Ilnam Kang,Yoon‐Joo Ko,Beomkoo Chung,Hyunsung Nam,Seokhee Kim,Kyuho Moon,Ki‐Bong Oh,Jang‐Cheon Cho,Sang Kook Lee,Dong‐Chan Oh
出处
期刊:Angewandte Chemie [Wiley]
卷期号:63 (21) 被引量:1
标识
DOI:10.1002/anie.202402465
摘要

Abstract A targeted metabologenomic method was developed to selectively discover terminal oxazole‐bearing natural products from bacteria. For this, genes encoding oxazole cyclase, a key enzyme in terminal oxazole biosynthesis, were chosen as the genomic signature to screen bacterial strains that may produce oxazole‐bearing compounds. Sixteen strains were identified from the screening of a bacterial DNA library (1,000 strains) using oxazole cyclase gene‐targeting polymerase chain reaction (PCR) primers. The PCR amplicon sequences were subjected to phylogenetic analysis and classified into nine clades. 1 H− 13 C coupled‐HSQC NMR spectra obtained from the culture extracts of the hit strains enabled the unequivocal detection of the target compounds, including five new oxazole compounds, based on the unique 1 J CH values and chemical shifts of oxazole: lenzioxazole ( 1 ) possessing an unprecedented cyclopentane, permafroxazole ( 2 ) bearing a tetraene conjugated with carboxylic acid, tenebriazine ( 3 ) incorporating two modified amino acids, and methyl‐oxazolomycins A and B ( 4 and 5 ). Tenebriazine displayed inhibitory activity against pathogenic fungi, whereas methyl‐oxazolomycins A and B ( 4 and 5 ) selectively showed anti‐proliferative activity against estrogen receptor‐positive breast cancer cells. This metabologenomic method enables the logical and efficient discovery of new microbial natural products with a target structural motif without the need for isotopic labeling.
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